A human protein hydroxylase that accepts D-residues

Hwanho Choi; Adam P. Hardy; Thomas M. Leissing; Rasheduzzaman Chowdhury; Yu Nakashima; Wei Ge; Marios Markoulides; John S. Scotti; Philip A. Gerken; Helen Thorbjornsrud; Dahye Kang; Sungwoo Hong; Joongoo Lee; Michael A. McDonough; Hwangseo Park; Christopher J. Schofield

doi:10.1038/s42004-020-0290-5

A human protein hydroxylase that accepts D-residues

Hwanho Choi, Adam P. Hardy, Thomas M. Leissing, Rasheduzzaman Chowdhury, Yu Nakashima, Wei Ge, Marios Markoulides, John S. Scotti, Philip A. Gerken, Helen Thorbjornsrud, Dahye Kang, Sungwoo Hong, Joongoo Lee, Michael A. McDonough, Hwangseo Park, Christopher J. Schofield^*

^*この論文の責任著者

和漢医薬学総合研究所研究開発部門資源開発分野（天然物創薬学領域）

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

10 被引用数 (Scopus)

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Factor inhibiting hypoxia-inducible factor (FIH) is a 2-oxoglutarate-dependent protein hydroxylase that catalyses C3 hydroxylations of protein residues. We report FIH can accept (D)- and (L)-residues for hydroxylation. The substrate selectivity of FIH differs for (D) and (L) epimers, e.g., (D)- but not (L)-allylglycine, and conversely (L)- but not (D)-aspartate, undergo monohydroxylation, in the tested sequence context. The (L)-Leu-containing substrate undergoes FIH-catalysed monohydroxylation, whereas (D)-Leu unexpectedly undergoes dihydroxylation. Crystallographic, mass spectrometric, and DFT studies provide insights into the selectivity of FIH towards (L)- and (D)-residues. The results of this work expand the potential range of known substrates hydroxylated by isolated FIH and imply that it will be possible to generate FIH variants with altered selectivities.

本文言語	英語
論文番号	52
ジャーナル	Communications Chemistry
巻	3
号	1
DOI	https://doi.org/10.1038/s42004-020-0290-5
出版ステータス	出版済み - 2020/12/01

ASJC Scopus 主題領域

化学一般
環境化学
生化学
材料化学

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title = "A human protein hydroxylase that accepts D-residues",

abstract = "Factor inhibiting hypoxia-inducible factor (FIH) is a 2-oxoglutarate-dependent protein hydroxylase that catalyses C3 hydroxylations of protein residues. We report FIH can accept (D)- and (L)-residues for hydroxylation. The substrate selectivity of FIH differs for (D) and (L) epimers, e.g., (D)- but not (L)-allylglycine, and conversely (L)- but not (D)-aspartate, undergo monohydroxylation, in the tested sequence context. The (L)-Leu-containing substrate undergoes FIH-catalysed monohydroxylation, whereas (D)-Leu unexpectedly undergoes dihydroxylation. Crystallographic, mass spectrometric, and DFT studies provide insights into the selectivity of FIH towards (L)- and (D)-residues. The results of this work expand the potential range of known substrates hydroxylated by isolated FIH and imply that it will be possible to generate FIH variants with altered selectivities.",

author = "Hwanho Choi and Hardy, {Adam P.} and Leissing, {Thomas M.} and Rasheduzzaman Chowdhury and Yu Nakashima and Wei Ge and Marios Markoulides and Scotti, {John S.} and Gerken, {Philip A.} and Helen Thorbjornsrud and Dahye Kang and Sungwoo Hong and Joongoo Lee and McDonough, {Michael A.} and Hwangseo Park and Schofield, {Christopher J.}",

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year = "2020",

month = dec,

day = "1",

doi = "10.1038/s42004-020-0290-5",

language = "英語",

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journal = "Communications Chemistry",

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T1 - A human protein hydroxylase that accepts D-residues

AU - Choi, Hwanho

AU - Hardy, Adam P.

AU - Leissing, Thomas M.

AU - Chowdhury, Rasheduzzaman

AU - Nakashima, Yu

AU - Ge, Wei

AU - Markoulides, Marios

AU - Scotti, John S.

AU - Gerken, Philip A.

AU - Thorbjornsrud, Helen

AU - Kang, Dahye

AU - Hong, Sungwoo

AU - Lee, Joongoo

AU - McDonough, Michael A.

AU - Park, Hwangseo

AU - Schofield, Christopher J.

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Factor inhibiting hypoxia-inducible factor (FIH) is a 2-oxoglutarate-dependent protein hydroxylase that catalyses C3 hydroxylations of protein residues. We report FIH can accept (D)- and (L)-residues for hydroxylation. The substrate selectivity of FIH differs for (D) and (L) epimers, e.g., (D)- but not (L)-allylglycine, and conversely (L)- but not (D)-aspartate, undergo monohydroxylation, in the tested sequence context. The (L)-Leu-containing substrate undergoes FIH-catalysed monohydroxylation, whereas (D)-Leu unexpectedly undergoes dihydroxylation. Crystallographic, mass spectrometric, and DFT studies provide insights into the selectivity of FIH towards (L)- and (D)-residues. The results of this work expand the potential range of known substrates hydroxylated by isolated FIH and imply that it will be possible to generate FIH variants with altered selectivities.

AB - Factor inhibiting hypoxia-inducible factor (FIH) is a 2-oxoglutarate-dependent protein hydroxylase that catalyses C3 hydroxylations of protein residues. We report FIH can accept (D)- and (L)-residues for hydroxylation. The substrate selectivity of FIH differs for (D) and (L) epimers, e.g., (D)- but not (L)-allylglycine, and conversely (L)- but not (D)-aspartate, undergo monohydroxylation, in the tested sequence context. The (L)-Leu-containing substrate undergoes FIH-catalysed monohydroxylation, whereas (D)-Leu unexpectedly undergoes dihydroxylation. Crystallographic, mass spectrometric, and DFT studies provide insights into the selectivity of FIH towards (L)- and (D)-residues. The results of this work expand the potential range of known substrates hydroxylated by isolated FIH and imply that it will be possible to generate FIH variants with altered selectivities.

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U2 - 10.1038/s42004-020-0290-5

DO - 10.1038/s42004-020-0290-5

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SN - 2399-3669

VL - 3

JO - Communications Chemistry

JF - Communications Chemistry

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ER -

A human protein hydroxylase that accepts D-residues

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